Table 4.
Active Therapeutic Clinical Trials for Patients with Leptomeningeal Metastases
| NCT | Phase | Primary Histology | Site, Sponsor | Drug | Primary Outcome(s) | Secondary Outcome(s) | Study Arms | Key Inclusion Criteria | Key Exclusion Criteria | Recruiting? |
|---|---|---|---|---|---|---|---|---|---|---|
| NCT02939300 | II | Melanoma | Massachusetts General Hospital, Bristol-Myers Squibb | Nivolumab and ipilimumab | OS | IC/EC RR LM RR IC/EC PFS Toxicity |
Single arm: combination of nivolumab with ipilimumab followed by nivolumab monotherapy | • Adults only • ECOG ≤2 or KPS ≥60 • Life expectancy ≥3 wks • LM confirmed by cytology |
• Active, known, or suspected autoimmune disease • Condition requiring systemic corticosteroid treatment • Prior systemic treatment with anti-CTLA4 antibody • Known history of active TB |
Yes |
| NCT01645839 | III | Breast cancer | Multiple sites in France, Centre Oscar Lambret | Liposomal cytarabine | Neurological PFS | Neurological, physical, cognitive, cytological, radiological improvement PFS (radiological, clinical, cytological) OS Toxicity |
A: Standard systemic treatment without liposomal cytarabine B: Standard systemic treatment with liposomal cytarabine |
• Female adults only • ECOG ≤2 • Life expectancy ≥2 mo • New diagnosis of LM by cytology OR clinical signs and symptoms • Measurable CNS disease < 0.5 cm or > 0.5 cm if focused radiation therapy |
• Symptomatic BM or BM requiring WBRT • Previous CSI or IT therapy • Previous systemic treatment with ARA-C or high-dose systemic methotrexate • Contraindication to LP and ventricular catheterization • VPS |
Yes |
| NCT01325207 | I/II | HER2+ breast cancer | Multiple US sites; Northwestern University | IT trastuzumab | Safety MTD |
Response (radiological, cytological, clinical) CSF PK |
Single arm, dose escalation: twice weekly for 2 wks, then weekly for 4 wks, then every 2 wks | • Adults only • HER2+ by IHC or FISH breast cancer • LM determined by MRI or cytology • Life expectancy ≥8 wks • KPS ≥50 • Willing to have Ommaya reservoir placed • May continue on IV trastuzumab, lapatinib or hormonal agents if controlling ECD and developed LM while on therapy |
• Previously-treated BM • BM requiring active treatment • Systemic agents (chemotherapy) that have CNS penetration, unless LM developed while on these agents and ECD controlled |
Ongoing, not recruiting |
| NCT01373710 | I/II | HER2+ breast cancer | Multiple sites in France, Institut Curie | IT/IVent trastuzumab | MTD | CNS TTP QoL OS PFS PK Radiological, CSF response |
Single arm, dose escalation: 1 injection/wk during 8 wks by lumbar puncture or Ommaya Reservoir, 4 dose levels expected from 30 mg to 150 mg | • Adults only • Life expectancy ≥2 mo • HER2+ by IHC and/or FISH • LM diagnosis by cytology and/or clinical signs and symptoms of LM with abnormal MRI |
• Symptomatic untreated BM • Symptomatic BM, unless surgery and/or RT were performed ≥3 wks before treatment initiation and lesion(s) accessible to IT or IVent treatment • Obstructive hydrocephalus • On lapatinib, unless wash out >2 wks before first dose of IT study drug • VPS or atrial shunt, unless can be turned off during treatment |
Yes |
| NCT02650752 | I | HER2+ breast cancer | 3 US sites, Memorial Sloan Kettering Cancer Center | High-dose lapatinib + capecitabine | MTD | Not specified | Single arm: weekly treatment cycle consisting of lapatinib 3 d on/11 d off + capecitabine 7 d on/7 d off. Both drugs administered orally with dose escalation. | • Female adults only • HER2+ by IHC or FISH • Life expectancy ≥12 wks • ECOG ≤2 • Non-escalating corticosteroid dose (≤16 mg dexamethasone daily) for ≥ 5 d • Radiological evidence of new and/or progressive BM/LM or CSF cytological evidence of LM |
• Prior capecitabine therapy allowed if ≥6 mo since last dose • Everolimus therapy • Craniotomy, other major surgery, open biopsy, or significant traumatic injury ≤4 wks of enrollment • HIV infection or chronic hepatitis B or C • Concurrent chemotherapy, hormonal therapy, radiation therapy, surgery, immunotherapy, tumor embolization, or biologic therapy, except for trastuzumab or hormonal therapy |
Yes |
| NCT02422641 | II | Breast cancer | Wake Forest University and Sidney Kimmel Comprehensive Cancer Center, Wake Forest University Health Sciences | High-dose methotrexate | 3 mo OS | 1 yr OS PFS Tolerability Cost Cytologic sterilization |
Single arm: high dose methotrexate (8 gm/m2 IV every 2 wks) | • Adults only • ECOG 0–1 • Triple negative, HER2+, or HR+ hormone refractory breast cancer • Cytologic or radiographic confirmation of LM with/without BM |
• Chemotherapy or SRS within 2 wks, WBRT within 6 mo • Heart failure (>NYHA Class 3) • Prior treatment with any methotrexate-containing systemic regimen within 1 yr (excluding IT methotrexate) • Concurrent or planned systemic chemotherapy, radiotherapy, or new hormonal/anti-HER2 directed therapy |
Yes |
| NCT02616393 | II | EGFR-mutant NSCLC | Multiple US sites, Kadmon Corp. LLC | Tesevatinib | Clinical activity using RECIST 1.1 (Cohorts A, C), symptom resolution (Cohort B) | QoL Median PFS CNS TTP Median OS PK |
Dosing the same among all arms: 300 mg orally once daily A: NSCLC who have progressed with BM B: NSCLC who have progressed with LM C: NSCLC with BM at initial presentation |
• Adults only • EGFR mutation that has clinical response to erlotinib, afatinib, or gefitinib • BM occurrence or progression while receiving erlotinib, afatinib, or gefitinib • Measurable BM (≥10 mm) • ECOG ≤2 • No clinically significant progression outside of the CNS on most recent EGFR inhibitor therapy |
• First day of dosing with tesevatinib • <2 wks from the last treatment of cytotoxic chemotherapy, biological therapy, or immunotherapy, • <6 wks for nitrosoureas and mitomycin C • <2 wks since surgical procedure • <4 wks since last CNS-direct RT • <3 d since discontinuing erlotinib, afatinib, or TKI • Any concurrent BM (Cohorts A and C), LM (Cohort B) therapy other than study treatment |
Yes |
| NCT02336451 | II | NSCLC with ALK rearrangement | Multiple US and international sites, Novartis | Ceritinib | ORR | TTIR and TTR IC/EC DOR IC/EC ORR IC/EC DCR PFS Safety PK |
Dosing the same among all arms: 750 mg orally once daily • ALK+ NSCLC with BM, without LM, with previous exposure to crizotinib • ALK+ NSCLC with BM, without LM, without previous exposure to crizotinib • ALK+ NSCLC with LM, with or without previous exposure to crizotinib |
• ≥1 measurable EC lesion • ECOG ≤2 • Life expectancy ≥6 wks |
• Prior ALK inhibitor other than crizotinib • BM requiring WBRT • Previously-treated BM, unless progressive or new since WBRT • Unstable or increasing dosage of corticosteroids • Planning to receive local treatment to BM (e.g. surgery, SRS, WBRT, IT chemotherapy) |
Yes |
| NCT00445965 | II | GD2-positive LMD (primarily neuroblastoma, primary CNS tumors) | Memorial Sloan Kettering Cancer Center, Same | IVent 131-I-labeled monoclonal antibody 3F8 | 6mo OS RR (alive at 6 mo) |
Toxicity | Single arm: 10 mCi injected IT weekly for up to 4 courses as tolerated | • Children and adults • Histologically-confirmed diagnosis of a malignancy known to express GD2 |
• Rapidly progressing or deteriorating neurologic examination • Obstructive or symptomatic communicating hydrocephalus • CSI or systemic chemotherapy <3 wks prior to start of protocol • >45 Gy CSI or >72 Gy focal brain radiation |
Ongoing, not recruiting |
| NCT00089245 | I | Malignancy known to be 8H9 reactive, confirmed by IHC or bone marrow IF | Memorial Sloan Kettering Cancer Center, Same | 131-I-labeled 8H9 | MTD over 2 yrs | Not specified | Single arm, dose escalation with patients entering in cohorts of: 3 patients at each dose level from 10–60 mCi 6 patients at each dose level from 70–100 mCi |
• Children and adults• LMD refractory to conventional therapies or recurrent brain tumors with predilection for LM dissemination (medulloblastoma, PNET, rhabdoid tumors) | • Rapidly progressing or deteriorating neurologic examination • Obstructive or symptomatic communicating hydrocephalus • CSI or systemic chemotherapy <3 wks prior to start of protocol |
Yes |
| NCT02308020 | II | HR+ breast cancer, NSCLC, or melanoma | Multiple US sites, Eli Lilly and Co. | Abemaciclib | IC ORR | BOIR IC DOR DCR IC DCR ICBR OS OR PFS PK at 3 mo |
Same treatment for all arms, UOS: 200mg study drug Q 12 hr, days 1–21 of each 21 d cycle • A: HER2+ breast cancer • B: HER2- breast cancer • C: Surgical resection indicated for intracranial lesions, drug days 5–14 prior to surgical resection and resumed dosing after wound healing • D: NSCLC, 150 mg drug if receiving concurrent gemcitabine or pemetrexed • E: Melanoma • F: HR+ Breast cancer, NSCLC, or melanoma |
• Adults only • KPS ≥70 • Life expectancy ≥12 wks • Completed local therapy (surgical resection, WBRT, or SRS) ≥14 d prior to initiating study drug |
• Require immediate local therapy (including WBRT, SRS, surgical resection) • Concurrent EIAED use • Evidence of symptomatic intracranial hemorrhage • ≥2 seizures within 4 wks prior to study initiation |
Yes |
| NCT02886585 | II | Multiple histologies | Massachusetts General Hospital, Merck Sharp & Dohme Corp. | Pembrolizumab | ORR OS EC ORR |
Toxicity OS rate IC/EC RR EC PFS |
Same treatment for all arms, UOS: study drug Q 3 wks • A: previously untreated BM • B: progressive BM after prior local CNS-directed therapy (e.g. WBRT, SRS, or surgery) • C: LM with positive CSF cytology • D: 1–4 BM from histologically-confirmed melanoma with clinical indication for SRS, cycles 1 and 2 of study drug administered 3 wks apart with SRS between |
• Adults only • Progressive systemic disease from any histologically or cytologically confirmed solid tumor • Measurable CNS disease (≥10 mm), except for Arm C • ECOG ≤2 or KPS ≥60 • Life expectancy ≥6 wks • Stable dose of dexamethasone ≤2 mg for ≥7 d prior to treatment initiation |
• Arm A: excludes HER2+ breast cancer, SCLC,; NSCLC with targetable genomic tumor aberrations (e.g. EGFR, ALK) • Known history of active TB • Immunodeficient HIV-positive participants on combination antiretroviral therapy • Prior treatment with an anti-PD-1, anti-PD-L1, or anti-PD-L2 agent |
Yes |
All information obtained from clinicaltrials.gov
Abbreviations:
ALK – anaplastic lymphoma kinase, BM – brain metastasis(es), BOIR – best overall intracranial response, CNS – central nervous system, CR – complete response, CSI – craniospinal irradiation, CTLA4 – Cytotoxic T-Lymphocyte Associated Protein 4, DCR – disease control rate, DOR – duration of response, EC – extracranial, ECD – extracranial disease, ECOG – Eastern Cooperative Oncology Group Performance Status, EGFR – epidermal growth factor receptor, EIAED – enzyme-inducing antiepileptic drugs, FISH – fluorescence in situ hybridization, HER2 – human epidermal growth factor receptor 2, HIV – human immunodeficiency virus, HR – hormone receptor, IC – intracranial, ICBR – intracranial clinical benefit rate, IF – immunofluorescence, IHC – immunohistochemistry, IT – intrathecal, IV – intravenous, IVent – intraventricular, KPS – Karnofsky Performance Status, LMD – leptomeningeal metastasis/disease, MTD – maximum tolerated dose, NSCLC – non-small cell lung cancer, NYHA – New York Heart Association, ORR – objective response rate, OS – overall survival, PD – progressive disease, PD/PD-L – Programmed Death/Programmed Death-Ligand, PFS – progression-free survival, PK – pharmacokinetics, QoL – quality of life, RR – response rate, RT – radiotherapy, SCLC – small cell lung cancer, SRS – stereotactic radiosurgery, TB – Bacillus Tuberculosis, TT(I)R – time to (intracranial) tumor response, TKI – tyrosine kinase inhibitor, TTP – time to progression, UOS – unless otherwise specified, VPS – ventriculoperitoneal shunt, WBRT – whole-brain radiation therapy